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评估荧光团连接的铂配合物以监测顺铂类似物的去向。

Evaluation of fluorophore-tethered platinum complexes to monitor the fate of cisplatin analogs.

作者信息

Jagodinsky Justin C, Sulima Agnieszka, Cao Yiqi, Poprawski Joanna E, Blackman Burchelle N, Lloyd John R, Swenson Rolf E, Gottesman Michael M, Hall Matthew D

机构信息

Laboratory of Cell Biology, National Cancer Institute, Center for Cancer Research, National Institutes of Health, 37 Convent Drive, Rm. 2108, Bethesda, MD, 20892, USA.

Imaging Probe Development Center, National Institutes of Health, Rockville, MD, USA.

出版信息

J Biol Inorg Chem. 2015 Oct;20(7):1081-95. doi: 10.1007/s00775-015-1290-2. Epub 2015 Sep 1.

Abstract

The platinum drugs cisplatin, carboplatin, and oxaliplatin are highly utilized in the clinic and as a consequence have been extensively studied in the laboratory setting, sometimes by generating fluorophore-tagged analogs. Here, we synthesized two Pt(II) complexes containing ethane-1,2-diamine ligands linked to a BODIPY fluorophore, and compared their biological activity with previously reported Pt(II) complexes conjugated to carboxyfluorescein and carboxyfluorescein diacetate. The cytotoxicity and DNA damage capacity of Pt-fluorophore complexes was compared to cisplatin, and the Pt-BODIPY complexes were found to be more cytotoxic with reduced cytotoxicity in cisplatin-resistant cells. Microscopy revealed a predominately cytosolic localization, with nuclear distribution at higher concentrations. Spheroids grown from parent and resistant cells revealed penetration of Pt-BODIPY into spheroids, and retention of the cisplatin-resistant spheroid phenotype. While most activity profiles were retained for the Pt-BODIPY complexes, accumulation in resistant cells was only slightly affected, suggesting that some aspects of Pt-fluorophore cellular pharmacology deviate from cisplatin.

摘要

铂类药物顺铂、卡铂和奥沙利铂在临床上得到了广泛应用,因此在实验室环境中也得到了广泛研究,有时是通过生成荧光团标记的类似物来进行研究。在此,我们合成了两种含有与BODIPY荧光团相连的乙二胺配体的Pt(II)配合物,并将它们的生物活性与先前报道的与羧基荧光素和羧基荧光素二乙酸酯共轭的Pt(II)配合物进行了比较。将Pt-荧光团配合物的细胞毒性和DNA损伤能力与顺铂进行了比较,发现Pt-BODIPY配合物具有更高的细胞毒性,而在顺铂耐药细胞中的细胞毒性降低。显微镜检查显示其主要定位于细胞质中,在较高浓度下有核分布。由亲本细胞和耐药细胞生长而成的球体显示Pt-BODIPY可穿透球体,并保留顺铂耐药球体的表型。虽然Pt-BODIPY配合物保留了大多数活性特征,但在耐药细胞中的积累仅受到轻微影响,这表明Pt-荧光团细胞药理学的某些方面与顺铂有所不同。

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